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拉克罗斯病毒的毒力受多基因控制。

Virulence of La Crosse virus is under polygenic control.

作者信息

Janssen R S, Nathanson N, Endres M J, Gonzalez-Scarano F

出版信息

J Virol. 1986 Jul;59(1):1-7. doi: 10.1128/JVI.59.1.1-7.1986.

Abstract

To identify which RNA segments of the California serogroup bunyaviruses determine virulence, we prepared reassortant viruses by coinfecting BHK-21 cells with two wild-type parents, La Crosse/original and Tahyna/181-57 viruses, which differed about 30,000-fold in virulence. The progeny clones were screened by polyacrylamide gel electrophoresis to ascertain the phenotype of the M and S RNA segments, and RNA-RNA hybridization was used to determine the genotype of selected clones. Two or three clones of each of the six possible reassortant genotypes were characterized quantitatively for neuroinvasiveness by determining the PFU/50% lethal dose (LD50) ratio after subcutaneous injection into suckling mice. The reassortants fell into two groups. (i) Six of seven reassortants with a La Crosse M RNA segment were as virulent as the parent La Crosse virus (about 1 PFU/LD50); the one exception was strikingly different (about 1,000 PFU/LD50) and probably represents a spontaneous mutant. (ii) The seven reassortants with a Tahyna M RNA segment were about 10-fold more virulent than the parent Tahyna virus (median 1,600 PFU/LD50 for reassortants and 16,000 PFU/LD50 for Tahyna virus). A comparative pathogenesis study in suckling mice of one reassortant virus and the parent Tahyna virus confirmed the greater neuroinvasiveness of the reassortant virus. From these data it was concluded that the M RNA segment was the major determinant of virulence, but that the other two gene segments could modulate the virulence of a nonneuroinvasive California serogroup virus.

摘要

为了确定加利福尼亚血清群布尼亚病毒的哪些RNA片段决定毒力,我们通过用两种野生型亲本病毒(拉克罗斯/原始病毒和塔伊纳/181 - 57病毒)共同感染BHK - 21细胞来制备重配病毒,这两种亲本病毒的毒力相差约30000倍。通过聚丙烯酰胺凝胶电泳筛选子代克隆,以确定M和S RNA片段的表型,并使用RNA - RNA杂交来确定所选克隆的基因型。通过测定皮下注射到乳鼠体内后的PFU/50%致死剂量(LD50)比值,对六种可能的重配基因型中的每一种的两到三个克隆进行了神经侵袭性的定量表征。重配病毒分为两组。(i)七个带有拉克罗斯M RNA片段的重配病毒中有六个与亲本拉克罗斯病毒一样具有毒力(约1 PFU/LD50);唯一的例外差异显著(约1000 PFU/LD50),可能代表一个自发突变体。(ii)七个带有塔伊纳M RNA片段的重配病毒的毒力比亲本塔伊纳病毒高约10倍(重配病毒的中位数为1600 PFU/LD50,塔伊纳病毒为16000 PFU/LD50)。对一种重配病毒和亲本塔伊纳病毒在乳鼠中的比较发病机制研究证实了重配病毒具有更强的神经侵袭性。从这些数据得出结论,M RNA片段是毒力的主要决定因素,但其他两个基因片段可以调节非神经侵袭性加利福尼亚血清群病毒的毒力。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/51a1/253030/c0b9b497b716/jvirol00106-0011-a.jpg

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